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肠道细菌丁酸生产肠单胞菌改善宿主代谢健康:队列研究和动物干预研究的证据

Gut bacterium Intestinimonas butyriciproducens improves host metabolic health: evidence from cohort and animal intervention studies.

作者信息

Rampanelli Elena, Romp Nadia, Troise Antonio Dario, Ananthasabesan Jakshana, Wu Hao, Gül Ismail Sahin, De Pascale Sabrina, Scaloni Andrea, Bäckhed Fredrik, Fogliano Vincenzo, Nieuwdorp Max, Bui Thi Phuong Nam

机构信息

Department of Experimental Vascular Medicine, Amsterdam UMC, Amsterdam, the Netherlands.

Amsterdam Institute for Immunology and Infectious Diseases, Amsterdam, the Netherlands.

出版信息

Microbiome. 2025 Jan 20;13(1):15. doi: 10.1186/s40168-024-02002-9.

Abstract

BACKGROUND

The human gut microbiome strongly influences host metabolism by fermenting dietary components into metabolites that signal to the host. Our previous work has shown that Intestinimonas butyriciproducens is a prevalent commensal bacterium with the unique ability to convert dietary fructoselysine to butyrate, a well-known signaling molecule with proven health benefits. Dietary fructoselysine is an abundant Amadori product formed in foods during thermal treatment and is part of foods rich in dietary advanced glycation end products which have been associated with cardiometabolic disease. It is therefore of interest to investigate the causal role of this bacterium and fructoselysine metabolism in metabolic disorders.

RESULTS

We assessed associations of I. butyriciproducens with metabolic risk biomarkers at both strain and functional levels using a human cohort characterized by fecal metagenomic analysis. We observed that the level of the bacterial strain as well as fructoselysine fermentation genes were negatively associated with BMI, triglycerides, HbA1c, and fasting insulin levels. We also investigated the fructoselysine degradation capacity within the Intestinimonas genus using a culture-dependent approach and found that I. butyriciproducens is a key player in the butyrogenic fructoselysine metabolism in the gut. To investigate the function of I. butyriciproducens in host metabolism, we used the diet-induced obesity mouse model to mimic the human metabolic syndrome. Oral supplementation with I. butyriciproducens counteracted body weight gain, hyperglycemia, and adiposity. In addition, within the inguinal white adipose tissue, bacterial administration reduced inflammation and promoted pathways involved in browning and insulin signaling. The observed effects may be partly attributable to the formation of the short-chain fatty acids butyrate from dietary fructoselysine, as butyrate plasma and cecal levels were significantly increased by the bacterial strain, thereby contributing to the systemic effects of the bacterial treatment.

CONCLUSIONS

I. butyriciproducens ameliorates host metabolism in the context of obesity and may therefore be a good candidate for new microbiota-therapeutic approaches to prevent or treat metabolic diseases. Video Abstract.

摘要

背景

人类肠道微生物群通过将饮食成分发酵成向宿主发出信号的代谢物,对宿主代谢产生强烈影响。我们之前的研究表明,丁酸生产肠单胞菌是一种常见的共生细菌,具有将饮食中的果糖赖氨酸转化为丁酸的独特能力,丁酸是一种具有已证实的健康益处的著名信号分子。饮食中的果糖赖氨酸是食物在热处理过程中形成的一种丰富的阿马多里产物,是富含饮食晚期糖基化终产物的食物的一部分,这些产物与心脏代谢疾病有关。因此,研究这种细菌和果糖赖氨酸代谢在代谢紊乱中的因果作用具有重要意义。

结果

我们使用通过粪便宏基因组分析表征的人类队列,在菌株和功能水平上评估了丁酸生产肠单胞菌与代谢风险生物标志物的关联。我们观察到细菌菌株水平以及果糖赖氨酸发酵基因与体重指数、甘油三酯、糖化血红蛋白和空腹胰岛素水平呈负相关。我们还使用依赖培养的方法研究了肠单胞菌属内的果糖赖氨酸降解能力,发现丁酸生产肠单胞菌是肠道中产丁酸的果糖赖氨酸代谢的关键参与者。为了研究丁酸生产肠单胞菌在宿主代谢中的功能,我们使用饮食诱导的肥胖小鼠模型来模拟人类代谢综合征。口服补充丁酸生产肠单胞菌可抵消体重增加、高血糖和肥胖。此外,在腹股沟白色脂肪组织中,给予细菌可减轻炎症并促进与褐变和胰岛素信号传导相关的途径。观察到的效果可能部分归因于饮食中的果糖赖氨酸形成短链脂肪酸丁酸,因为该细菌菌株使血浆和盲肠中的丁酸水平显著升高,从而有助于细菌治疗的全身效应。

结论

丁酸生产肠单胞菌在肥胖背景下改善宿主代谢,因此可能是预防或治疗代谢疾病的新型微生物治疗方法的良好候选者。视频摘要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b363/11744835/528b30af4d34/40168_2024_2002_Fig1_HTML.jpg

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